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Cdc7 kinase - A new target for drug development

  • Ronan Swords
  • , Devalingam Mahalingam
  • , Michael O'Dwyer
  • , Corrado Santocanale
  • , Kevin Kelly
  • , Jennifer Carew
  • , Francis Giles
  • University of Texas Health Science Center San Antonio
  • Galway University Hospital

Research output: Contribution to a Journal (Peer & Non Peer)Articlepeer-review

71 Citations (Scopus)

Abstract

The cell division cycle 7 (Cdc7) is a serine threonine kinase that is of critical importance in the regulation of normal cell cycle progression. Cdc7 kinase is highly conserved during evolution and much has been learned about its biological roles in humans through the study of lower eukaryotes, particularly yeasts. Two important regulator proteins, Dbf4 and Drf1, bind to and modulate the kinase activity of human Cdc7 which phosphorylates several sites on Mcm2 (minichromosome maintenance protein 2), one of the six subunits of the replicative DNA helicase needed for duplication of the genome. Through regulation of both DNA synthesis and DNA damage response, both key functions in the survival of tumour cells, Cdc7 becomes an attractive target for pharmacological inhibition. There are much data available on the pre-clinical anti-cancer effects of Cdc7 depletion and although there are no available Cdc7 inhibitors in clinical trials as yet, several lead compounds are being optimised for this purpose. In this review, we will address the current status of Cdc7 as an important target for new drug development.

Original languageEnglish
Pages (from-to)33-40
Number of pages8
JournalEuropean Journal of Cancer
Volume46
Issue number1
DOIs
Publication statusPublished - 1 Jan 2010

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

  1. SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well-being

Keywords

  • Cdc7 kinase
  • Cell cycle
  • Drug development
  • Target

Authors (Note for portal: view the doc link for the full list of authors)

  • Authors
  • Swords R, Mahalingam D, O'Dwyer M, Santocanale C, Kelly K, Carew J, Giles F
  • Swords, R. and Mahalingam, D. and O'Dwyer, M. and Santocanale, C. and Kelly, K. and Carew, J. and Giles, F.

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